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转录组学证据表明,从烟草转向电子烟并不能逆转对呼吸道上皮的损害。

Transcriptomic Evidence That Switching from Tobacco to Electronic Cigarettes Does Not Reverse Damage to the Respiratory Epithelium.

作者信息

Pozuelos Giovanna L, Kagda Meenakshi, Rubin Matine A, Goniewicz Maciej L, Girke Thomas, Talbot Prue

机构信息

Department of Molecular, Cell and Systems Biology, University of California, Riverside, CA 92521, USA.

Department of Health Behavior, Roswell Park Comprehensive Cancer Center, Buffalo, NY 14203, USA.

出版信息

Toxics. 2022 Jul 4;10(7):370. doi: 10.3390/toxics10070370.

Abstract

The health benefits of switching from tobacco to electronic cigarettes (ECs) are neither confirmed nor well characterized. To address this problem, we used RNA-seq analysis to compare the nasal epithelium transcriptome from the following groups ( = 3 for each group): (1) former smokers who completely switched to second generation ECs for at least 6 months, (2) current tobacco cigarette smokers (CS), and (3) non-smokers (NS). Group three included one former cigarette smoker. The nasal epithelial biopsies from the EC users vs. NS had a higher number of differentially expressed genes (DEGs) than biopsies from the CS vs. NS and CS vs. EC sets (1817 DEGs total for the EC vs. NS, 407 DEGs for the CS vs. NS, and 116 DEGs for the CS vs. EC comparison). In the EC vs. NS comparison, enriched gene ontology terms for the downregulated DEGs included cilium assembly and organization, whereas gene ontologies for upregulated DEGs included immune response, keratinization, and NADPH oxidase. Similarly, ontologies for cilium movement were enriched in the downregulated DEGs for the CS vs. NS group. Reactome pathway analysis gave similar results and also identified keratinization and cornified envelope in the upregulated DEGs in the EC vs. NS comparison. In the CS vs. NS comparison, the enriched Reactome pathways for upregulated DEGs included biological oxidations and several metabolic processes. Regulator effects identified for the EC vs. NS comparison were inflammatory response, cell movement of phagocytes and degranulation of phagocytes. Disease Ontology Sematic Enrichment analysis identified lung disease, mouth disease, periodontal disease and pulmonary fibrosis in the EC vs. NS comparison. Squamous metaplasia associated markers, keratin 10, keratin 13 and involucrin, were increased in the EC vs. NS comparison. Our transcriptomic analysis showed that gene expression profiles associated with EC use are not equivalent to those from non-smokers. EC use may interfere with airway epithelium recovery by promoting increased oxidative stress, inhibition of ciliogenesis, and maintaining an inflammatory response. These transcriptomic alterations may contribute to the progression of diseases with chronic EC use.

摘要

从烟草转向电子烟(EC)对健康的益处尚未得到证实,也未得到充分描述。为了解决这个问题,我们使用RNA测序分析来比较以下几组(每组n = 3)的鼻上皮转录组:(1)完全改用第二代电子烟至少6个月的 former smokers,(2)当前的烟草吸烟者(CS),以及(3)非吸烟者(NS)。第三组包括一名 former cigarette smoker。与NS相比,EC使用者的鼻上皮活检中差异表达基因(DEG)的数量高于CS与NS以及CS与EC组的活检(EC与NS相比共有1817个DEG,CS与NS相比有407个DEG,CS与EC相比有116个DEG)。在EC与NS的比较中,下调DEG的富集基因本体术语包括纤毛组装和组织,而上调DEG的基因本体包括免疫反应、角化和NADPH氧化酶。同样,纤毛运动的本体在CS与NS组的下调DEG中富集。Reactome通路分析给出了类似的结果,并且在EC与NS的比较中上调DEG中也鉴定出了角化和角质化包膜。在CS与NS的比较中,上调DEG的富集Reactome通路包括生物氧化和几个代谢过程。EC与NS比较确定的调节因子效应是炎症反应、吞噬细胞的细胞运动和吞噬细胞的脱颗粒。疾病本体语义富集分析在EC与NS的比较中鉴定出了肺部疾病、口腔疾病、牙周疾病和肺纤维化。在EC与NS的比较中,鳞状化生相关标志物角蛋白10、角蛋白13和内披蛋白增加。我们的转录组分析表明,与使用EC相关的基因表达谱与非吸烟者的不同。使用EC可能通过促进氧化应激增加、抑制纤毛发生和维持炎症反应来干扰气道上皮的恢复。这些转录组改变可能导致长期使用EC引发疾病的进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/55a0/9321508/9e3b394f66c8/toxics-10-00370-g001.jpg

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